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Global assessment of Mycobacterium avium subsp. hominissuis genetic requirement for growth and virulence

Abstract

Nontuberculous mycobacterial infections caused by the opportunistic pathogen Mycobacterium avium subsp. hominissuis (MAH) are currently receiving renewed attention due to increased incidence combined with difficult treatment. Insights into the disease-causing mechanisms of this species have been hampered by difficulties in genetic manipulation of the bacteria. Here, we identified and sequenced a highly transformable, virulent MAH clinical isolate susceptible to high-density transposon mutagenesis, facilitating global gene disruption and subsequent investigation of MAH gene function. By transposon insertion sequencing (TnSeq) of this strain, we defined the MAH genome-wide genetic requirement for virulence and in vitro growth and organized ∼3,500 identified transposon mutants for hypothesis-driven research. The majority (96%) of the genes we identified as essential for MAH in vitro had a mutual ortholog in the related and highly virulent Mycobacterium tuberculosis (Mtb). However, passaging our library through a mouse model of infection revealed a substantial number (54% of total hits) of novel virulence genes. More than 97% of the MAH virulence genes had a mutual ortholog in Mtb. Finally, we validated novel genes required for successful MAH infection: one encoding a probable major facilitator superfamily (MFS) transporter and another encoding a hypothetical protein located in the immediate vicinity of six other identified virulence genes. In summary, we provide new, fundamental insights into the underlying genetic requirement of MAH for growth and host infection.
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Category

Academic article

Language

English

Author(s)

  • Marte Singsås Dragset
  • Thomas R. Ioerger
  • Maja Loevenich
  • Markus Haug
  • Niruja Sivakumar
  • Anne Marstad
  • Pere-Joan Cardona
  • Geir Klinkenberg
  • Eric J. Rubin
  • Magnus Steigedal
  • Trude Helen Flo

Affiliation

  • SINTEF Industry / Biotechnology and Nanomedicine
  • Germans Trias i Pujol Research Institute
  • St. Olavs Hospital, Trondheim University Hospital
  • Norwegian University of Science and Technology
  • Texas A&M University-College Station
  • Harvard School of Public Health

Year

2019

Published in

mSystems

Volume

4

Issue

6

Page(s)

1 - 16

View this publication at Norwegian Research Information Repository